The generation of stable microvessels in ischemia is mediated by endothelial cell derived TRAIL

Siân P. Cartland; Manisha S. Patil; Elaina Kelland; Natalie Le; Lauren Boccanfuso; Christopher P. Stanley; Pradeep Manuneedhi Cholan; Malathi I. Dona; Ralph Patrick; Jordan McGrath; Qian Peter Su; Imala Alwis; Ruth Ganss; Joseph E. Powell; Richard P. Harvey; Alexander R. Pinto; Thomas S. Griffith; Jacky Loa; Sarah J. Aitken; David A. Robinson; Sanjay Patel; Mary M. Kavurma

doi:10.1126/sciadv.adn8760

The generation of stable microvessels in ischemia is mediated by endothelial cell derived TRAIL

Siân P. Cartland
, Manisha S. Patil
, Elaina Kelland
, Natalie Le
, Lauren Boccanfuso
, Christopher P. Stanley
, Pradeep Manuneedhi Cholan
, Malathi I. Dona
, Ralph Patrick
, Jordan McGrath
, Qian Peter Su
, Imala Alwis
, Ruth Ganss
, Joseph E. Powell
, Richard P. Harvey
, Alexander R. Pinto
, Thomas S. Griffith
, Jacky Loa
, Sarah J. Aitken
, David A. Robinson

Sanjay Patel, Mary M. Kavurma

UWA Centre for Medical Research (affiliated with the Harry Perkins Institute of Medical Research)

Research output: Contribution to journal › Article › peer-review

9 Citations (Web of Science)

Abstract

Reversal of ischemia is mediated by neo-angiogenesis requiring endothelial cell (EC) and pericyte interactions to form stable microvascular networks. We describe an unrecognized role for tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) in potentiating neo-angiogenesis and vessel stabilization. We show that the endothelium is a major source of TRAIL in the healthy circulation compromised in peripheral artery disease (PAD). EC deletion of TRAIL in vivo or in vitro inhibited neo-angiogenesis, pericyte recruitment, and vessel stabilization, resulting in reduced lower-limb blood perfusion with ischemia. Activation of the TRAIL receptor (TRAIL-R) restored blood perfusion and stable blood vessel networks in mice. Proof-of-concept studies showed that Conatumumab, an agonistic TRAIL-R2 antibody, promoted vascular sprouts from explanted patient arteries. Single-cell RNA sequencing revealed heparin-binding EGF-like growth factor in mediating EC-pericyte communications dependent on TRAIL. These studies highlight unique TRAIL-dependent mechanisms mediating neo-angiogenesis and vessel stabilization and the potential of repurposing TRAIL-R2 agonists to stimulate stable and functional microvessel networks to treat ischemia in PAD.

Original language	English
Article number	eadn8760
Number of pages	17
Journal	Science Advances
Volume	10
Issue number	40
DOIs	https://doi.org/10.1126/sciadv.adn8760
Publication status	Published - 4 Oct 2024

Funding

Funders	Funder number
NHMRC National Health and Medical Research Council	2028501, 1188218, 1188503, 2021463

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Cartland, S. P., Patil, M. S., Kelland, E., Le, N., Boccanfuso, L., Stanley, C. P., Cholan, P. M., Dona, M. I., Patrick, R., McGrath, J., Su, Q. P., Alwis, I., Ganss, R., Powell, J. E., Harvey, R. P., Pinto, A. R., Griffith, T. S., Loa, J., Aitken, S. J., ... Kavurma, M. M. (2024). The generation of stable microvessels in ischemia is mediated by endothelial cell derived TRAIL. Science Advances, 10(40), Article eadn8760. https://doi.org/10.1126/sciadv.adn8760

@article{be4fdf0a4aa8409087843bcfc0f55e0a,

title = "The generation of stable microvessels in ischemia is mediated by endothelial cell derived TRAIL",

abstract = "Reversal of ischemia is mediated by neo-angiogenesis requiring endothelial cell (EC) and pericyte interactions to form stable microvascular networks. We describe an unrecognized role for tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) in potentiating neo-angiogenesis and vessel stabilization. We show that the endothelium is a major source of TRAIL in the healthy circulation compromised in peripheral artery disease (PAD). EC deletion of TRAIL in vivo or in vitro inhibited neo-angiogenesis, pericyte recruitment, and vessel stabilization, resulting in reduced lower-limb blood perfusion with ischemia. Activation of the TRAIL receptor (TRAIL-R) restored blood perfusion and stable blood vessel networks in mice. Proof-of-concept studies showed that Conatumumab, an agonistic TRAIL-R2 antibody, promoted vascular sprouts from explanted patient arteries. Single-cell RNA sequencing revealed heparin-binding EGF-like growth factor in mediating EC-pericyte communications dependent on TRAIL. These studies highlight unique TRAIL-dependent mechanisms mediating neo-angiogenesis and vessel stabilization and the potential of repurposing TRAIL-R2 agonists to stimulate stable and functional microvessel networks to treat ischemia in PAD.",

author = "Cartland, \{Si{\^a}n P.\} and Patil, \{Manisha S.\} and Elaina Kelland and Natalie Le and Lauren Boccanfuso and Stanley, \{Christopher P.\} and Cholan, \{Pradeep Manuneedhi\} and Dona, \{Malathi I.\} and Ralph Patrick and Jordan McGrath and Su, \{Qian Peter\} and Imala Alwis and Ruth Ganss and Powell, \{Joseph E.\} and Harvey, \{Richard P.\} and Pinto, \{Alexander R.\} and Griffith, \{Thomas S.\} and Jacky Loa and Aitken, \{Sarah J.\} and Robinson, \{David A.\} and Sanjay Patel and Kavurma, \{Mary M.\}",

year = "2024",

month = oct,

day = "4",

doi = "10.1126/sciadv.adn8760",

language = "English",

volume = "10",

journal = "Science Advances",

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Cartland, SP, Patil, MS, Kelland, E, Le, N, Boccanfuso, L, Stanley, CP, Cholan, PM, Dona, MI, Patrick, R, McGrath, J, Su, QP, Alwis, I, Ganss, R, Powell, JE, Harvey, RP, Pinto, AR, Griffith, TS, Loa, J, Aitken, SJ, Robinson, DA, Patel, S & Kavurma, MM 2024, 'The generation of stable microvessels in ischemia is mediated by endothelial cell derived TRAIL', Science Advances, vol. 10, no. 40, eadn8760. https://doi.org/10.1126/sciadv.adn8760

TY - JOUR

T1 - The generation of stable microvessels in ischemia is mediated by endothelial cell derived TRAIL

AU - Cartland, Siân P.

AU - Patil, Manisha S.

AU - Kelland, Elaina

AU - Le, Natalie

AU - Boccanfuso, Lauren

AU - Stanley, Christopher P.

AU - Cholan, Pradeep Manuneedhi

AU - Dona, Malathi I.

AU - Patrick, Ralph

AU - McGrath, Jordan

AU - Su, Qian Peter

AU - Alwis, Imala

AU - Ganss, Ruth

AU - Powell, Joseph E.

AU - Harvey, Richard P.

AU - Pinto, Alexander R.

AU - Griffith, Thomas S.

AU - Loa, Jacky

AU - Aitken, Sarah J.

AU - Robinson, David A.

AU - Patel, Sanjay

AU - Kavurma, Mary M.

PY - 2024/10/4

Y1 - 2024/10/4

N2 - Reversal of ischemia is mediated by neo-angiogenesis requiring endothelial cell (EC) and pericyte interactions to form stable microvascular networks. We describe an unrecognized role for tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) in potentiating neo-angiogenesis and vessel stabilization. We show that the endothelium is a major source of TRAIL in the healthy circulation compromised in peripheral artery disease (PAD). EC deletion of TRAIL in vivo or in vitro inhibited neo-angiogenesis, pericyte recruitment, and vessel stabilization, resulting in reduced lower-limb blood perfusion with ischemia. Activation of the TRAIL receptor (TRAIL-R) restored blood perfusion and stable blood vessel networks in mice. Proof-of-concept studies showed that Conatumumab, an agonistic TRAIL-R2 antibody, promoted vascular sprouts from explanted patient arteries. Single-cell RNA sequencing revealed heparin-binding EGF-like growth factor in mediating EC-pericyte communications dependent on TRAIL. These studies highlight unique TRAIL-dependent mechanisms mediating neo-angiogenesis and vessel stabilization and the potential of repurposing TRAIL-R2 agonists to stimulate stable and functional microvessel networks to treat ischemia in PAD.

AB - Reversal of ischemia is mediated by neo-angiogenesis requiring endothelial cell (EC) and pericyte interactions to form stable microvascular networks. We describe an unrecognized role for tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) in potentiating neo-angiogenesis and vessel stabilization. We show that the endothelium is a major source of TRAIL in the healthy circulation compromised in peripheral artery disease (PAD). EC deletion of TRAIL in vivo or in vitro inhibited neo-angiogenesis, pericyte recruitment, and vessel stabilization, resulting in reduced lower-limb blood perfusion with ischemia. Activation of the TRAIL receptor (TRAIL-R) restored blood perfusion and stable blood vessel networks in mice. Proof-of-concept studies showed that Conatumumab, an agonistic TRAIL-R2 antibody, promoted vascular sprouts from explanted patient arteries. Single-cell RNA sequencing revealed heparin-binding EGF-like growth factor in mediating EC-pericyte communications dependent on TRAIL. These studies highlight unique TRAIL-dependent mechanisms mediating neo-angiogenesis and vessel stabilization and the potential of repurposing TRAIL-R2 agonists to stimulate stable and functional microvessel networks to treat ischemia in PAD.

UR - https://www.scopus.com/pages/publications/85205788184

U2 - 10.1126/sciadv.adn8760

DO - 10.1126/sciadv.adn8760

M3 - Article

C2 - 39365855

AN - SCOPUS:85205788184

SN - 2375-2548

VL - 10

JO - Science Advances

JF - Science Advances

IS - 40

M1 - eadn8760

ER -

The generation of stable microvessels in ischemia is mediated by endothelial cell derived TRAIL

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